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首页> 外文期刊>Journal of clinical laboratory analysis. >Endothelin‐1 rs9296344 associates with the susceptibility of childhood primary nephrotic syndrome
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Endothelin‐1 rs9296344 associates with the susceptibility of childhood primary nephrotic syndrome

机译:内皮素-1 rs9296344与儿童原发性肾病综合征的易感性相关联

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摘要

Background Recently, the rs5370 single nucleotide polymorphisms (SNPs) of Endothelin‐1 ( EDN1) showed association with the susceptibility of childhood primary nephrotic syndrome (CPNS). This study aims to investigate potential relationships between other EDN1 SNPs and CPNS. Methods Seven SNPs (rs5370, rs10478723, rs1476046, rs1800541, rs2070698, rs2071942, and rs9296344) of the EDN1 gene were genotyped in 579 CPNS patients and 586 age‐matched healthy children. Then, we analyzed potential associations of the six SNPs with susceptibility of CPNS by using rs5370 as a conditional variant in a logistic regression model. SNP‐SNP interaction analysis was performed to investigate the joint effects of the seven SNPs in the pathogenesis of CPNS. Results Independent with rs5370, only rs9296344 significantly associated (T vs C, odds ratio [OR] = 0.71, 95% confidence interval [CI] = 0.57‐0.88, P =?.001) with the susceptibility of CPNS. Meanwhile, no joint effect among the analyzed seven SNPs was discovered in this study. Conclusions This study discovered that C allele of rs9296344 on EDN1 is a novel independent risk factor for CPNS.
机译:背景技术最近,内皮素-1(EDN1)的RS5370单核苷酸多态性(SNP)显示与儿童原发性肾病综合征(CPNS)的敏感性相关性。本研究旨在调查其他EDN1 SNP和CPNS之间的潜在关系。方法七个SNP(RS5370,RS10478723,RS1476046,RS1800541,RS2070698,RS2071942和RS9296344)在579名CPNS患者和586岁的健康儿童中进行基因分型。然后,我们通过使用RS5370作为逻辑回归模型中的条件变体,分析了六个SNP的潜在关联。进行SNP-SNP相互作用分析以研究七个SNP在CPNS发病机制中的关节效应。结果与RS5370无关,只有RS9296344显着相关(T VS C,差距[或] = 0.71,95%置信区间[CI] = 0.57-0.88,P =Δ001),具有CPNS的易感性。同时,在本研究中发现了分析的七个SNP中没有关节效应。结论本研究发现,EDN1上的RS9296344的C等位基因是CPNS的新型独立危险因素。

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